Differential Interferon Responses Enhance Viral Epitope Generation by Myocardial Immunoproteasomes in Murine Enterovirus Myocarditis

Sandra J?kel; Ulrike Kuckelkorn; Gudrun Szalay; Michael Pl?tz; Kathrin Textoris-Taube; Elisa Opitz; Karin Klingel; Stefan Stevanovic; Reinhard Kandolf; Katja Kotsch; Karl Stangl; Peter M. Kloetzel; Antje Voigt

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Differential Interferon Responses Enhance Viral Epitope Generation by Myocardial Immunoproteasomes in Murine Enterovirus Myocarditis

机译：差异性干扰素反应增强小鼠肠病毒性心肌炎中心肌免疫蛋白酶体的病毒表位生成

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Murine models of coxsackievirus B3 (CVB3)-induced myocarditis mimic the divergent human disease course of cardiotropic viral infection, with host-specific outcomes ranging from complete recovery in resistant mice to chronic disease in susceptible hosts. To identify susceptibility factors that modulate the course of viral myocarditis, we show that type-I interferon (IFN) responses are considerably impaired in acute CVB3-induced myocarditis in susceptible mice, which have been linked to immunoproteasome (IP) formation. Here we report that in concurrence with distinctive type-I IFN kinetics, myocardial IP formation peaked early after infection in resistant mice and was postponed with maximum IP expression concomitant to massive inflammation and predominant type-II IFN responses in susceptible mice. IP activity is linked to a strong enhancement of antigenic viral peptide presentation. To investigate the impact of myocardial IPs in CVB3-induced myocarditis, we identified two novel CVB3 T cell epitopes, virus capsid protein 2 [285-293] and polymerase 3D [2170-2177]. Analysis of myocardial IPs in CVB3-induced myocarditis revealed that myocardial IP expression resulted in efficient epitope generation. As opposed to the susceptible host, myocardial IP expression at early stages of disease corresponded to enhanced CVB3 epitope generation in the hearts of resistant mice. We propose that this process may precondition the infected heart for adaptive immune responses. In conclusion, type-I IFN-induced myocardial IP activity at early stages coincides with less severe disease manifestation in CVB3-induced myocarditis.

机译：柯萨奇病毒B3（CVB3）诱导的心肌炎的小鼠模型 >在易感的宿主中抵抗慢性疾病的抗性小鼠的恢复。为了确定调节病毒性心肌炎病程的易感性因素，我们证明了在急性CVB3诱导的中，I型干扰素（IFN）的反应明显受损。 sup>易感小鼠的心肌炎，与免疫蛋白酶（IP）的形成有关。在这里，我们报告说，与独特的 I型IFN动力学同时，抗感染小鼠的心肌IP形成在感染后早期达到峰值，并被最大IP 表达伴随大量炎症和主要的 II型IFN应答。 IP活性与与抗原性病毒肽呈递作用的增强有关。为了研究心肌IP在CVB3诱导的心肌炎中的影响，我们确定了两个新的CVB3 T细胞表位，病毒衣壳蛋白2 [285-293]和聚合酶3D [2170-2177]。对CVB3诱发的心肌炎中心肌IP的分析显示，心肌IP表达可产生有效的表位。与易感宿主相反，心肌IP疾病早期的表达对应于抗性小鼠心脏中增强的CVB3表位生成。我们建议这个过程可以为感染的心脏提供适应性的免疫应答的先决条件。总之，在CVB3诱发的心肌炎中，I型IFN诱发的心肌IP活性在早期与疾病的严重程度较低的表现相吻合。

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《American Journal of Pathology》 |2009年第2期|510-518|共9页
作者
Sandra J?kel; Ulrike Kuckelkorn; Gudrun Szalay; Michael Pl?tz; Kathrin Textoris-Taube; Elisa Opitz; Karin Klingel; Stefan Stevanovic; Reinhard Kandolf; Katja Kotsch; Karl Stangl; Peter M. Kloetzel; Antje Voigt;
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From the Institute for Biochemistry,Charité-Universit?tsmedizin Berlin, Berlin;

From the Institute for Biochemistry,Charité-Universit?tsmedizin Berlin, Berlin;

the Department of Molecular Pathology,University Hospital, Tuebingen;

and the Clinic for Cardiology and Angiology,Campus Mitte, Charité-Universit?tsmedizin Berlin, Berlin;

From the Institute for Biochemistry,Charité-Universit?tsmedizin Berlin, Berlin;

and the Clinic for Cardiology and Angiology,Campus Mitte, Charité-Universit?tsmedizin Berlin, Berlin;

the Department of Molecular Pathology,University Hospital, Tuebingen;

the Department of Molecular Pathology,University Hospital, Tuebingen;

the Department of Molecular Pathology,University Hospital, Tuebingen;

and the Clinic for Immunology,Charité-Universit?tsmedizin Berlin, Berlin;

and the Clinic for Cardiology and Angiology,Campus Mitte, Charité-Universit?tsmedizin Berlin, Berlin;

From the Institute for Biochemistry,Charité-Universit?tsmedizin Berlin, Berlin;

and the Clinic for Cardiology and Angiology,Campus Mitte, Charité-Universit?tsmedizin Berlin, Berlin;

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1. Differential interferon responses enhance viral epitope generation by myocardial immunoproteasomes in murine enterovirus myocarditis. [J] . Jakel S, Kuckelkorn U, Szalay G American Journal of Pathology: Official Publication of the American Association of Pathologists . 2009,第2期

机译：差异性干扰素反应可增强鼠肠病毒心肌炎中心肌免疫蛋白酶体的病毒表位生成。
2. Leptin deficiency enhances myocardial necrosis and lethality in a murine model of viral myocarditis. [J] . Kanda T, Takahashi T, Kudo S, Life sciences . 2004,第12期

机译：瘦素缺乏会在病毒性心肌炎的小鼠模型中增强心肌坏死和致死率。
3. Impairment of Immunoproteasome Function by β5i/LMP7 Subunit Deficiency Results in Severe Enterovirus Myocarditis [J] . Anna Rahnefeld, Annett Koch, Antje Voigt, PLoS Pathogens . 2011,第9期

机译：β5i/ LMP7亚基缺陷对免疫蛋白酶体功能的损害导致严重肠病毒性心肌炎
4. The value of Radionuclide Myocardial Perfusion Imaging in children with viral myocarditis [C] . Xiaomei Zhang, Qianqian Wang, Delei Zhang, International Symposium on Information Technologies in Medicine and Education;ITME 2012 . 2012

机译：放射性核素心肌灌注显像在病毒性心肌炎患儿中的价值
5. Targeted deletion of Fgl2 enhances anti-viral T cell responses and mediates viral clearance in a murine model of chronic viral infection [D] . Luft, Olga 2014

机译：针对FL1的靶向缺失增强了抗病毒T细胞应答并在慢性病毒感染的小鼠模型中介导病毒清除
6. Differential Interferon Responses Enhance Viral Epitope Generation by Myocardial Immunoproteasomes in Murine Enterovirus Myocarditis [O] . Sandra Jäkel, Ulrike Kuckelkorn, Gudrun Szalay, 2009

机译：差异性干扰素反应增强小鼠肠病毒性心肌炎中心肌免疫蛋白酶体的病毒表位生成
7. Differential Interferon Responses Enhance Viral Epitope Generation by Myocardial Immunoproteasomes in Murine Enterovirus Myocarditis [O] . Jäkel, Sandra, Kuckelkorn, Ulrike, Szalay, Gudrun, 2009

机译：差异性干扰素反应增强小鼠肠病毒性心肌炎中心肌免疫蛋白酶体的病毒表位生成

Differential Interferon Responses Enhance Viral Epitope Generation by Myocardial Immunoproteasomes in Murine Enterovirus Myocarditis

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